A20, a modulator of smooth muscle cell proliferation and apoptosis, prevents and induces regression of neointimal hyperplasia

Patel, Virendra I.; Daniel, Soizic; Longo, Christopher R.; Shrikhande, Gautam; Scali, Salvatore T.; Czismadia, Eva; Groft, Caroline M.; Shukri, Tala; Motley-Dore, Christina; Ramsey, Haley E.; Fisher, Mark D.; Grey, Shane T.; Arvelo, Maria B.; Ferran, Christiane

doi:10.1096/fj.05-4981com

Cited by 69 publications

(70 citation statements)

References 52 publications

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“…One caveat of this conclusion is that our studies determining the relative activities of FVB-A20 and B6-A20 were done in transfected 293 and vascular smooth muscle cells, whereas in the current study A20 in lesions was localized mainly to endothelial cells and lipid-laden macrophages. Although unlikely, it is possible that A20 mediates different functions (antiapoptotic vs. NF-B activation) in these cell types so that in sum the FVB form could be proatherogenic (33,34). Thus it will be necessary to study cell type-specific conditional knockdown of A20 before entirely excluding it as the responsible atherosclerosis susceptibility gene at the chromosome 10 locus.…”

Section: Discussionmentioning

confidence: 99%

The protective effect of A20 on atherosclerosis in apolipoprotein E-deficient mice is associated with reduced expression of NF-κB target genes

Wolfrum

Teupser

Tan

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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Up-regulation of inflammatory responses is considered a driving force of atherosclerotic lesion development. One key regulator of inflammation is the A20 (also called TNF-␣-induced protein 3 or Tnfaip3) gene, which is responsible for NF-B termination and maps to an atherosclerosis susceptibility locus revealed by quantitative trait locus-mapping studies at mouse proximal chromosome 10. In the current study, we examined the role of A20 in atherosclerotic lesion development. At the aortic root lesion size was found to be increased in C57BL/6 (BG) apolipoprotein E-deficient (ApoE ؊/؊ ) mice haploinsufficient for A20, compared with B6 ApoE ؊/؊ controls that expressed A20 normally (60% in males and 23% in females; P < 0.001 and P < 0.05, respectively). In contrast, lesion size was found to be decreased in F 1 (B6؋FVB/N) mice overexpressing A20 by virtue of containing an A20 BAC transgene compared with nontransgenic controls (30% in males, P < 0.001, and 17% in females, P ‫؍‬ 0.02). The increase in lesions in the A20 haploinsufficient mice correlated with increased expression of proatherosclerotic NF-B target genes, such as vascular cell adhesion molecule 1, intercellular adhesion molecule 1, and macrophage-colony-stimulating factor, and elevated plasma levels of NF-B-driven cytokines. These findings suggest that A20 diminishes atherosclerosis by decreasing NF-B activity, thereby modulating the proinflammatory state associated with lesion development.A therosclerosis is a chronic inflammatory disease influenced by many genes, and mouse models are useful for identifying these genes and determining their mechanisms of action. We previously carried out an intercrosses between atherosclerosissensitive apolipoprotein E-deficient (ApoE Ϫ/Ϫ ) C57BL/6 (B6) and atherosclerosis-resistant ApoE Ϫ/Ϫ FVB mice, and by quantitative trait locus mapping identified an atherosclerosissusceptibility locus on proximal chromosome 10 (1, 2). A candidate gene in this region, A20, encodes a broadly expressed cytoplasmic protein that inhibits both TNF-␣-and IL-1␤/Tolllike receptor (TLR)-induced NF-B activation through mediating the destruction of receptor-interacting serine/threonine protein kinase 1 (RIP) and TNF receptor-associated factor 6 in their respective signaling complexes (3, 4). Up-regulation of NF-B activity leads to increased expression of many genes with established roles in atherosclerosis, including cytokines, chemokines, adhesion molecules, acute phase proteins, and regulators of apoptosis and cell proliferation. NF-B terminates its own activation by inducing the expression of I B␣ and A20. A20-deficient (A20 Ϫ/Ϫ ) mice die prematurely because of cachexia and spontaneous inflammation in several organs. This phenotype correlates with the failure to properly terminate TNF-induced NF-B activity in fibroblasts isolated from A20 Ϫ/Ϫ mice (5). We previously determined that A20 derived from B6 and FVB mice differs in a single amino acid residue (E627A; B6 vs. FVB). We showed this finding to be functionally significant by demonstrating...

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Section: Discussionmentioning

confidence: 99%

The protective effect of A20 on atherosclerosis in apolipoprotein E-deficient mice is associated with reduced expression of NF-κB target genes

Wolfrum

Teupser

Tan

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

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“…In SMC, NF-κB is essential for the acquisition of a pro-inflammatory SMC phenotype, promoting migration into the neointima, proliferation and leukocytes migration into TV lesions. Concommitant to NF-κB activation, A20 inhibits the subsequent up-regulation of proatherogenic NF-κB dependent genes such as ICAM-1 and MCP-1 and also A20 SMC proliferation via increased expression of the cyclin dependent kinase inhibitors p21 waf1 and p27 kip1 (12) . Further, we demonstrate that A20 expression in SMC results in sensitization to cytokine and Fas mediated apoptosis through a novel NO-dependent mechanism.…”

Section: Discussionmentioning

confidence: 99%

“…We have evidence that he 7Zn finger protein A20 is part of the protective phenotype of the vessel wall against TV. A20 is a NF-κB dependent stress response gene in EC and SMC with potent antiinflammatory effect in both cell types through blockade of NF-κB (11,12 ). However, its effect on apoptosis is rather cell type and stimulus specific.…”

Section: Introductionmentioning

confidence: 99%

The Universal NF-kappaB Inhibitor A20 Protects From Transplant Vasculopathy by Differentially Affecting Apoptosis in Endothelial and Smooth Muscle Cells

Daniel

Patel

Shrikhande

et al. 2006

Transplantation Proceedings

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Transplant vasculopathy (TV) is an accelerated form of atherosclerosis resulting in chronic rejection of vascularized allografts. The causes of TV are multifactorial and integrate at the level of the vascular wall, leading to a phenotypic switch of endothelial (EC) and smooth muscle cells (SMC). A20 is a NF-κB dependent stress response gene in EC and SMC with potent anti-inflammatory effect in both cell types through blockade of NF-κB. A20 expression in EC and SMC correlates with the absence of TV in rat kidney allografts and long term functioning human kidney allografts.We demonstrate that A20 protects EC from TNF, Fas and NK cell-mediated apoptosis by inhibiting proteolytic cleavage of caspase 8. A20 also safeguards EC from complement-mediated necrosis. Hence, effectively shutting down cell death pathways initiated by inflammatory and immune offenders associated with TV.In contrast, A20 sensitizes SMC to cytokine and Fas mediated apoptosis through a novel nitric oxide (NO)-dependent mechanism. The unexpected pro-apoptotic effect of A20 in SMC translates in vivo by the regression of established neointimal carotid lesions following balloon angioplasty in rats. Antedating apoptosis of SMC, expression of the inducible nitric oxide synthase increases in A20 expressing neointimal SMC, corroborating the involvement of NO in causing the pro-apoptotic effect of A20 in SMC.Combined anti-inflammatory and anti or pro-apoptotic functions of A20 in EC and SMC respectively qualify the positive effect of A20 upon vascular remodeling and healing. We propose that A20 based therapies may be effective in prevention and treatment of TV.

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“…In VSMCs transfected with A20, expression of p53 and the p53 target genes p21 waf1 and p27 kip is increased [85], which would be expected to contribute to the anti-proliferative effect of A20. The effect of A20-deficiency on cell proliferation has not yet been tested, which is essential to confirm that A20 regulates cell proliferation under physiological conditions.…”

Section: 5other Functions Of A20 (See Table 2)mentioning

confidence: 99%

Expression, biological activities and mechanisms of action of A20 (TNFAIP3)

Verstrepen

Verhelst

Loo

et al. 2010

Biochemical Pharmacology

174

152

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A20 (also known as TNFAIP3) is a cytoplasmic protein that plays a key role in the negative regulation of inflammation and immunity. Polymorphisms in the A20 gene locus have been identified as risk alleles for multiple human autoimmune diseases, and A20 has also been proposed to function as a tumor suppressor in several human B-cell lymphomas. A20 expression is strongly induced by multiple stimuli, including the proinflammatory cytokines TNF and IL-1, and microbial products that trigger pathogen recognition receptors, such as Toll-like receptors. A20 functions in a negative feedback loop, which mediates its inhibitory functions by downregulating key proinflammatory signaling pathways, including those controlling NF-κB-and IRF3-dependent gene expression. Activation of these transcription factors is controlled by both K48-and K63-polyubiquitination of upstream signaling proteins, respectively triggering proteasome-mediated degradation or interaction with other signaling proteins. A20 turns off NF-B and IRF3 activation by modulating both types of ubiquitination. Induction of K48-polyubiquitination by A20 involves its C-terminal zincfinger ubiquitin-binding domain, which may promote interaction with E3 ligases, such as Itch and RNF11 that are involved in mediating A20 inhibitory functions. A20 is thought to promote de-ubiquitination of K63-polyubiquitin chains either directly, due to its N-terminal deubiquitinase domain, or by disrupting the interaction between E3 and E2 enzymes that catalyze K63-polyubiquitination. A20 is subject to different mechanisms of regulation, including phosphorylation, proteolytic processing, and association with ubiquitin binding proteins. Here we review the expression and biological activities of A20, as well as the underlying molecular mechanisms.

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A20, a modulator of smooth muscle cell proliferation and apoptosis, prevents and induces regression of neointimal hyperplasia

Cited by 69 publications

References 52 publications

The protective effect of A20 on atherosclerosis in apolipoprotein E-deficient mice is associated with reduced expression of NF-κB target genes

The protective effect of A20 on atherosclerosis in apolipoprotein E-deficient mice is associated with reduced expression of NF-κB target genes

The Universal NF-kappaB Inhibitor A20 Protects From Transplant Vasculopathy by Differentially Affecting Apoptosis in Endothelial and Smooth Muscle Cells

Expression, biological activities and mechanisms of action of A20 (TNFAIP3)

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